2009
DOI: 10.1080/15257770903316145
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Activity of siRNAs with 2-Thio-2′-O-Methyluridine Modification in Mammalian Cells

Abstract: In a search to identify chemical modifications to improve the properties of siRNA, we have investigated the effect of the 2 '-O-methyl-2-thiouridine modification on the biological activity of siRNA. Our results indicate that judicious placement of 2 '-O-methyl-2-thiouridine residues could lead to modified siRNA with activity in mammalian cells.

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Cited by 6 publications
(4 citation statements)
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“…In most cases, activating PKR is an unwanted side effect. High translation and low immunogenicity make mRNA containing Ψ or m5C applicable to express therapeutic proteins, whereas s2U-modified RNA is best suited for applications where avoiding nonspecific immunogenicity is desirable but where translation is unnecessary (33), such as delivering antisense RNA (55) or stimulating RNA interference.…”
Section: Discussionmentioning
confidence: 99%
“…In most cases, activating PKR is an unwanted side effect. High translation and low immunogenicity make mRNA containing Ψ or m5C applicable to express therapeutic proteins, whereas s2U-modified RNA is best suited for applications where avoiding nonspecific immunogenicity is desirable but where translation is unnecessary (33), such as delivering antisense RNA (55) or stimulating RNA interference.…”
Section: Discussionmentioning
confidence: 99%
“…Although nucleoside suppressors of both TLR3 and TLR7/8 have been described (Karikó, Buckstein, Ni, & Weissman, 2005) (Table 1), their impact on siRNA-mediated TLR3 activation has not been assessed. Presently, reports on the impact of 2-thiouridine on slicer function are contradictory (Prakash, Naik, Sioufi, Bhat, & Swayze, 2009;Sipa et al, 2007). Overall, judicious use of one or two 2' modified nucleosides as formulation adjuncts (e.g.…”
Section: Sirna and Mirna Mediated Immune Responsesmentioning
confidence: 99%
“…The solid supports of this family have successfully been applied in the synthesis of natural oligoribonucleotides and their 2 -F-analogs (Prakash et al, 2005(Prakash et al, , 2009Tedebark et al, 2011, Lima et al, 2012, LNA oligonucleotides (Ravikumar et al, 2008), oligonucleotides containing 2 ,4 -(Nmethoxy)aminomethylene-, 2 ,4 -aminooxymethylene-, and 2 -O,4 -C-aminomethylenebridged nucleoside analogs (Prakash et al, 2010), and oxepane and 2 -enopyranose nucleoside analogs (Sabatino and Damha, 2007).…”
Section: 112mentioning
confidence: 99%